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首页> 外文期刊>Ecological indicators >Carboxylesterase in Spams aurata: Characterisation and sensitivity to organophosphorus pesticides and pharmaceutical products
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Carboxylesterase in Spams aurata: Characterisation and sensitivity to organophosphorus pesticides and pharmaceutical products

机译:垃圾邮件光环中的羧基酯酶:对有机磷农药和医药产品的表征和敏感性

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Organophosphorus (OP) and carbamate (CB) pesticides cause inhibition of acetylcholinesterase (AChE, which is the target enzyme) and carboxylesterase (CbE). However, some studies have suggested that CbE could have a potential protective role on AChE since CbE seems to be more sensitive to the inhibition by OP and CB compounds than the target enzyme. In addition, there is a great deal of concern about the presence of pharmaceutical products in the seas, and some studies have pointed out the utility of CbE as a biomarker and scavenger of them. Thus, our main aim was to study the inhibition caused by the OPs chlorpyrifos-oxon (CP-O) and dichlorvos (DCV), and the carbamate eserine on the hepatic CbE and the brain AChE of Sparus aurata. Another goal was to determine the hepatic CbE inhibition caused by ibuprofen, fenofibrate, simvastatin, carbamazepine, and triclosan. To achieve these goals, we studied the localisation of CbE in Sparus aurata and estimated the kinetic parameters of hepatic CbE. The results of this study indicate that most CbE activity occurs in the plasma and liver. However, the kinetic parameters of hepatic CbE measured on the three substrates used appeared to be very similar. Hepatic CbE was more sensitive to DCV than brain AChE, suggesting a possible protective role of CbE on AChE. Finally, CbE was shown to be sensitive to the inhibition caused by triclosan and simvastatin, indicating its utility as a biomarker and as a scavenger of these compounds to reduce the possible adverse effects on the organisms.
机译:有机磷(OP)和氨基甲酸酯(CB)农药引起对乙酰胆碱酯酶(AChE,它是目标酶)和羧酸酯酶(CbE)的抑制作用。但是,一些研究表明CbE可能对AChE具有潜在的保护作用,因为CbE似乎比目标酶对OP和CB化合物的抑制作用更为敏感。此外,人们对海洋中存在的药品存在很多担忧,一些研究指出了CbE作为它们的生物标记和清除剂的效用。因此,我们的主要目的是研究OPs毒死rif(CP-O)和Dichlorvos(DCV)以及氨基甲酸酯色氨酸对Sparus aurata肝CbE和脑AChE的抑制作用。另一个目标是确定由布洛芬,非诺贝特,辛伐他汀,卡马西平和三氯生引起的肝CbE抑制作用。为了实现这些目标,我们研究了Spabura aurata中CbE的定位并估算了肝脏CbE的动力学参数。这项研究的结果表明,大多数CbE活性发生在血浆和肝脏中。但是,在所用的三种底物上测得的肝CbE动力学参数似乎非常相似。肝CbE对DCV的敏感性高于脑AChE,表明CbE对AChE可能具有保护作用。最后,CbE已显示出对三氯生和辛伐他汀引起的抑制作用敏感,表明其可作为生物标志物和这些化合物的清除剂以减少对生物体的不利影响。

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